APT also reports the
Science
time and
Total Charged
time (including overheads)
for your observation on the line labeled
Duration
. Note that this is an observation-level assessment, and only includes overheads internal to the observation. You will see these fields update as you enter and change parameters in the observation specification. Finally, although is is not in a gray box, APT reports the
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it ascribes to the observation. This is for information only and also updates as changes are made to the observation specification.

For observing modes that require information for a target acquisition, the observation template contains a labeledsection for this information (see Figure 2). The observation specifications for the target acquisition should be brought forward from an appropriate
ETC calculation
.

Various science parameters in an observing template are entered in a panel in the lower half of the observation form in the active GUI window. This section usually has up to four tabs;

Users can leave and return to a given observation
template
as many times as needed as they iterate various options in their proposal preparation. Red X's indicate errors, which might indicate something as simple as missing information or improperly specified parameters that need to be corrected. Once an observation
template
is cleared of errors, it can be run through the
Visit Planner
to check its schedulability.

In the APTtree editor, there's an item called
Observation Links
. It
contains
an overall summary of any and all
special requirements
specified for linking observations in the proposal. This provides a way to
quickly verify whether the links have been set as intended, and is particularly useful if you have specified repeated observations that should be similar to each other.

The signs and symptoms of low blood sugar can vary depending on the person and how quickly the level falls. Also, problems other than hypoglycemia or diabetes
can cause similar symptoms.

Warning signs of low blood sugar include:

Kidswho have nocturnal hypoglycemia may have bouts of crying, nightmares, or night sweats (with damp sheets and/or pajamas), and might wake up groggy or with a headache.

When blood sugar levels fall too low, the body releases the hormone adrenaline, which helps get stored glucose into the bloodstream quickly. Paleness, sweating, shakiness, and increased heart rate are early warning signs of this adrenaline release.

More severe symptoms — such as confusion, drowsiness, seizures, and loss of consciousness —
may happen i
f the hypoglycemia isn't treated and
the brain doesn't get enough glucose to work properly.

The only way to know for sure if your child has low blood sugar levels is to test them.
Blood sugar levels can be tested with a
glucose meter
, a computerized device that measures and displays the amount of glucose in a blood sample. However, if the situation makes it impossible or inconvenient to quickly check the blood sugar, it's important to treat your child for hypoglycemia immediately to prevent symptoms from getting worse.

The only way to know for sure if your child has low blood sugar levels is to test them.

Sometimes a child with diabetes may have symptoms of low blood sugar, but the levels are not actually low. This is a called a
false reaction
. Adrenaline also can be released when blood sugar levels fall rapidly from a high level to a normal level. Testing blood sugar levels before giving treatment for hypoglycemia can help you identify false reactions.

false reaction

Also, some kids may learn to fake symptoms of low blood sugar to get a sugary treat or avoid something unpleasant. Again, checking the blood sugar level can confirm the presence of hypoglycemia.

It's important to discuss the signs and symptoms of low blood sugar with your child. Even younger kids who can't verbalize symptoms should learn how to alert their parents when they don't feel well. This will help kids make the connection between how they feeland the need for treatment. Kids also should know when and how to find an adult for help.

Some people with diabetes don't have or can't sense the early warning signs of low blood sugar, a condition known as
hypoglycemic unawareness
. They're at greater risk for not recognizing the need to get treatment for hypoglycemia promptly. This could lead to more serious symptoms, such as loss of consciousness or seizures, as their blood sugar falls.

Increased production of the proinflammatory cytokine TNF-α is associated with obesity-related insulin resistance
39
as well as obesity-related hypertension.
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In rats, TNF-α elevation concomitantly impairs insulin-mediated muscle capillary recruitment and glucose uptake.
4,19
In addition, in humans, circulating TNF-α levels are associated with reduced whole body glucose uptake and skin capillary recruitment.
39
In isolated skeletal muscle resistance arteries, we could demonstrate that TNF-α impairs the vasodilator effects but not the vasoconstrictor effects of insulin through activation of intracellular enzyme c-Jun N-terminal kinase (JNK) and impairment of insulin-mediated activation of Akt.
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This selective inhibition of the vasodilator effects of insulin results in insulin-mediated vasoconstriction in the presence of TNF-α. JNK has been shown to regulate whole-body insulin sensitivity as well as insulin-mediated cell signaling.
42
In conclusion, both FFAs and TNF-α are likely candidates to link visceral adipose tissue with defects in microvascular function, at least in part by influencing insulin signaling and thereby the vascular effects of insulin.

We have recently hypothesized an alternative communicative pathway between adipose tissue and the microvasculature.
43
Obese Zucker rats are characterized by a well-circumscribed depot of fat cells around the origin of the nutritive arteriole supplying the cremaster muscle whereas lean rats are not. Adipokines released by these fat cells may directly inhibit vasodilatory pathways distal in the arteriole and thereby cause loss of blood flow in the nutritive capillary network supplied by this arteriole. In this hypothesis, which remains to be tested, adipokines released from periarteriolar fat depots have a local rather than a systemic vasoregulatory effect, which we named “vasocrine”.

Arterial stiffness has recently been recognized as an important cardiovascular risk factor.
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All classic risk factors, including age, hypertension, diabetes, smoking, and low-density lipoprotein (LDL) cholesterol, are determinants of arterial stiffness. In the Atherosclerosis Risk in Communities Study, the fasting insulin concentration was positively correlated with several indexes of arterial stiffness.
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This relationship was independent of age, cigarette-years, and cholesterol and suggested, assuming fasting hyperinsulinemia to be a marker of insulin resistance, that insulin resistance may contribute to stiffening of large arteries. Indeed, subsequent cross sectional epidemiological data suggest that insulin resistance and arterial stiffness are related.
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Moreover, the metabolic syndrome is associated with an increased progression of aortic stiffness with age.
47
In addition, insulin has direct effects on large arteries resulting in decreased augmentation of central aortic pressure as a result of reduced pulse wave reflection from the periphery.
48
This hemodynamic effect of insulin is blunted in obese insulin-resistant subjects
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and positively associated with insulin-mediated glucose uptake.
50
Unlike the effect of insulin on peripheral resistance vessels, which occurs only after a number of hours and at supraphysiological doses, the effect of insulin on arterial stiffness occurs rapidly and well within the physiological range comparable to insulin’s effects on the microcirculation.

Carefully
run the following commands; this will remove Android Studio and its related preferences and library files. This is the best way to completely uninstall Android Studio and prep it for reinstallation, if desired.